Leveraging antigenic seniority for maternal vaccination to prevent mother-to-child transmission of HIV-1

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作者
Ashley N. Nelson
Maria Dennis
Jesse F. Mangold
Katherine Li
Pooja T. Saha
Kenneth Cronin
Kaitlyn A. Cross
Amit Kumar
Riley J. Mangan
George M. Shaw
Katharine J. Bar
Barton Haynes
Anthony M. Moody
S. Munir Alam
Justin Pollara
Michael G. Hudgens
Koen K. A. Van Rompay
Kristina De Paris
Sallie R. Permar
机构
[1] Duke University Medical Center,Human Vaccine Institute
[2] University of North Carolina at Chapel Hill,Gillings School of Public Health and Center for AIDS Research
[3] Duke University School of Medicine,Molecular Genetics and Microbiology
[4] University of Pennsylvania,Department of Medicine
[5] University of California,California National Primate Research Center
[6] University of North Carolina at Chapel Hill,Department of Microbiology and Immunology and Center for AIDS Research, School of Medicine
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The development of a maternal HIV vaccine to synergize with current antiretroviral drug prophylaxis can overcome implementation challenges and further reduce mother-to-child transmission (MTCT) of HIV. Both the epitope-specificity and autologous neutralization capacity of maternal HIV envelope (Env)-specific antibodies have been implicated in decreased risk of MTCT of HIV. Our goal was to determine if heterologous HIV Env immunization of SHIV.C.CH505-infected, ART-suppressed female rhesus macaques (RMs) could boost autologous Env-specific antibodies. SHIV.C.CH505-infected female RMs (n = 12), began a daily ART regimen at 12 weeks post-infection (wpi), which was continued for 12 weeks. Starting 2 weeks after ART initiation, RMs received 3 monthly immunizations with HIV b.63521/1086.C gp120 or placebo (n = 6/group) vaccine with adjuvant STR8S-C. Compared to the placebo-immunized animals, Env-vaccinated, SHIV-infected RMs exhibited enhanced IgG binding, avidity, and ADCC responses against the vaccine immunogens and the autologous SHIV.C.CH505 Env. Notably, the Env-specific memory B cells elicited by heterologous vaccination were dominated by cells that recognized the SHIV.C.CH505 Env, the antigen of primary exposure. Thus, vaccination of SHIV-infected, ART-suppressed RMs with heterologous HIV Envs can augment multiple components of the antibody response against the Env antigen of primary exposure, suggesting antigenic seniority. Our results suggest that a universal maternal HIV vaccination regimen can be developed to leverage antigenic seniority in targeting the maternal autologous virus pool.
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